Registration for a live webinar on 'Precision medicine treatment for anticancer drug resistance' is now open.
See webinar detailsWe noted you are experiencing viewing problems
-
Check with your IT department that JWPlatform, JWPlayer and Amazon AWS & CloudFront are not being blocked by your network. The relevant domains are *.jwplatform.com, *.jwpsrv.com, *.jwpcdn.com, jwpltx.com, jwpsrv.a.ssl.fastly.net, *.amazonaws.com and *.cloudfront.net. The relevant ports are 80 and 443.
-
Check the following talk links to see which ones work correctly:
Auto Mode
HTTP Progressive Download Send us your results from the above test links at access@hstalks.com and we will contact you with further advice on troubleshooting your viewing problems. -
No luck yet? More tips for troubleshooting viewing issues
-
Contact HST Support access@hstalks.com
-
Please review our troubleshooting guide for tips and advice on resolving your viewing problems.
-
For additional help, please don't hesitate to contact HST support access@hstalks.com
We hope you have enjoyed this limited-length demo
This is a limited length demo talk; you may
login or
review methods of
obtaining more access.
Printable Handouts
Navigable Slide Index
- Introduction
- General properties of cancer cells
- Common tumors
- Human breast cancer tissue (1)
- Targeted mAbs to the ErbB2-Neu oncogene
- Amino acid sequences of forms of Neu protein
- Molecular assemblies
- Neu gene versus the normal form of the gene
- Consequence of mutation in ErbB2-Neu gene
- Outcome of over expression of 1 or 2 members
- Tyrosine phosphorylation patterns of Neu
- Dimerization analysis of ErbB receptors
- Over-expressed Neu & EGFR - malignancy
- Neu and EGFR: experiments in vivo
- ErbB3 and ErbB4 onco-proteins
- Resting and activated states of ErbB receptors
- EGFR conformations
- Molecular model of EGFR dimer
- A model of a kinase complex
- Signaling leads to activation of other machines
- Pathways are initiated when ErbB's form dimers
- Dimer formation by ErbB-R initiates signaling
- Early breast lesions over express receptors
- Additional overview: mAbs development
- Growth patterns of B104.1.1 and NIH3T3 cells
- Transformed cells by Neu gene: growth patterns
- ErbB2-Neu/Herceptin complex: crystal structure
- Use of the mAbs Herceptin
- Improved efficacy of two Abs to two epitopes
- Example: use of two Abs
- Herceptin and Omnitarg
- X-Ray crystalography of various Abs
- Prevention of reoccurence
- Frequency of tumours in mAb treated mice
- Herceptin in a preventative mode
- How do Abs affect malignant properties?
- Monovalent and bivalent Abs: loss of ErbB2-Neu
- Tetrameric species
- Tetrameric association of ErbB receptors (1)
- Tetrameric association of ErbB receptors (2)
- Cancer cells: more genetically abnormal
- Survivin characteristics
- The crystal structure of survivin
- Survivin acts through the ErbB-R stimulation
- ΔEGFR enhances survivin levels in U87MG cells
- Survivin levels affect cells vitality & proliferation
- Evolution of the cancer cell
- Human breast cancer tissue (2)
- Disabling onco-proteins with targeted mAbs (1)
- Disabling onco-proteins with targeted mAbs (2)
- Targeted mAbs limit survival of aneuploidic cells
- Disabling ErbB receptors by antibody treatment
- SKBR3 cells treated with 4D5 for seven days
- Herceptin qualities: summary
- Recent research
Topics Covered
- General properties of tumor cells
- Human breast cancer and the erbB2/neu oncogene and protein
- Targeted monoclonal antibodies
- Tyrosine kinase activity and dimerization
- Activation of the kinase of erbB2/neu
- Overexpression of erbB2/neu and EGFr
- The erbB family members
- Discussion of Herceptin
- Prevention of tumor growth in a neoadjuvant model
- Two antibody therapy & tumor growth inhibition
Links
Series:
Categories:
Therapeutic Areas:
Talk Citation
Greene, M. (2019, February 27). Monoclonal antibodies and the ErbB system in human cancer [Video file]. In The Biomedical & Life Sciences Collection, Henry Stewart Talks. Retrieved December 22, 2024, from https://doi.org/10.69645/QCWL3801.Export Citation (RIS)
Publication History
Financial Disclosures
- Prof. Mark Greene has not informed HSTalks of any commercial/financial relationship that it is appropriate to disclose.
A selection of talks on Immunology & Inflammation
Transcript
Please wait while the transcript is being prepared...
0:04
We will discuss the development of monoclonal antibodies
against the products of the ErbB family oncogenes.
The ErbB family of oncogenes have been implicated in a variety of human cancers,
and the development of monoclonal antibodies against
the ErbB2-Neu onco-protein represented
the first rational targeted therapy against human cancer.
Before we consider how cancer cells are affected my monoclonal antibodies,
we must discuss the differences between cancer cells and normal cells.
Cancer cells have growth independence from growth factors.
That is, growth factors normally are reliant on a variety of signals to keep them alive.
Cancer cells often become independent of this.
In the same way, cancer cells resist cell death on
a situation while normal cells die such as deprivation of nutrients.
Finally, cancer cells can undergo chromosomal alterations
and a stepwise change from less to more malignant cell types.
All of these features,
acquisition of growth independence,
resistance to cell death,
and progressive chromosomal alterations can be affected by
specific targeted disabling of onco-proteins involved in transformation of cells.
1:15
A variety of common tumors have abnormalities of the ErbB family of proteins.
Today, we'll concentrate on breast cancer,
a very common tumor in the United States.
Approximately 25-30 percent of breast cancers have abnormalities of
the ErbB2-Neu oncogene and abnormal expression of the ErbB2-Neu onco-protein.
Other common tumors such as lung cancer also have
abnormalities of ErbB oncogenes including the EGF receptor.
This tumor is particularly lethal,
and strategies to disable the EGF receptor may have some significant benefit.